Your search keyword '"T. Baroni"' showing total 117 results

1. Outstation for x-ray powder diffraction at the Italian beamline at the European synchrotron

Author

G. O. Lepore, S. Checchia, T. Baroni, M. Brunelli, and F. d’Acapito

Subjects

X-Ray Diffraction, X-Rays, Powders, Instrumentation, Synchrotrons, Powder Diffraction

Abstract

LISA [ Linea Italiana per la Spettroscopia di Assorbimento X, Italian beamline for X-ray Absorption Spectroscopy (XAS)] is the Italian CRG ( Collaborating Research Group) beamline at the ESRF ( European Synchrotron Radiation Facility) dedicated to XAS [d’Acapito et al., J. Synchrotron Radiat. 26, 551–558 (2019)]. In this work, a methodical test of the LISA beamline in performing diffraction measurements is carried out. Synchrotron x-ray diffraction measurements would complement absorption spectroscopy techniques with the long-range characterization of the material under investigation, while XAS provides the short-range element selective information.

Published

2022

2. Lung regions differently modulate bronchial branching development and extracellular matrix plays a role in regulating the development of chick embryo whole lung

Author

G Stabellini, M Calvitti, E Becchetti, P Carinci, C Calastrini, C Lilli, R Solmi, L Vizzotto, and T Baroni

Subjects

Biology (General), QH301-705.5

Abstract

Normal branching development is dependent on the correlation between cells and extracellular matrix. In this interaction glycosaminoglycans, cytokines and growth factors play a fundamental role. In order to verify the distribution and influence of extracellular matrix and related enzymes on chick embryo lung development, 6 day-old whole lungs were maintained in vitro with testicular hyaluronidase, b-N-acetyl-Dglucosaminidase and chondrotinase ABC or in linkage with apical, medial and caudal lung regions of 6-day development before and after enzyme treatment. In a separate lung region b-N-acetyl-D-glucosaminidase and hyaluronidase were determined. Our data show that the whole lung cultures increase bronchial branching development when the medial region is admixed separately, while the separate apical or caudal regions or apical combined with caudal region do not affect bronchial branching development. The enzyme treatment of medial region prevents the branching development in associated whole lung. The bronchial branching development of whole lung cultured in medium containing the enzymes related to glycosaminoglycans turnover is significantly altered. In conclusion, these data show that the different influence of separate apical, medial, caudal lung regions on bronchial branching development is related to the extracellular matrix composition.

Published

2009

3. Selective Enzymatic Debridement For The Management Of Acute Upper Limb Burns

Author

M, Cherubino, L, Valdatta, T, Baroni, I, Pellegatta, F, Tamborini, L, Garutti, P, Di Summa, and R, Adani

Subjects

Research Article

Abstract

Upper limb burn treatment represents a major medical and surgical challenge. Enzymatic escharolysis is a rather new technique to treat thermal burns in an easy and rapid way, as an alternative to the standard of care. The aim of the study was to investigate and describe the efficacy of treatment of upper limb burns with NexoBrid® in a non-burn referral center. All patients suffering from upper limb burns and admitted within 36 hours to the Hand and Microsurgery Unit of the ASST Sette Laghi from December 2016 to June 2018 were enrolled in the study. A retrospective analysis was performed, evaluating time to wound healing, time of hospitalization, and scar aesthetic appearance with patient and observer scar assessment scale (POSAS) and disabilities of the arm, shoulder and hand score (DASH). A total of 18 patients with burns involving the upper limb from December 2016 to June 2018 were treated. The mean TBSA% involved was 3%; 4 out of 18 patients suffered circumferential burns. The mean POSAS score was 14; the mean DASH score at 6-month follow up was 21, while it reduced to 11 at the last follow up visit. Enzymatic escharolysis is a novel, rapid and selective treatment option that allows early physiotherapy with overall satisfying functional results. We believe that enzymatic escharolysis should be considered, in most cases, as the standard of care in the treatment of upper limb burn wounds in non-burn referral centers.Le traitement des brûlures du membre supérieur (MS) est un défi médico- chirurgical majeur. Le débridement enzymatique est une technique relativement récente, facile et rapide, représentant une alternative au traitement classique. Le but de cette étude est d’évaluer l’utilisation du Nexobrid® dans le traitement, hors CTB, des brûlures du MS. Les 18 patients souffrant de brûlure du MS, hospitalisés entre décembre 2016 et juin 2018 dans le service de microchirurgie et de chirurgie de la main du Groupement Hospitalier de Territoire Sette Laghi dans les 36 h suivant l’accident ont été étudiés selon une étude rétrospective évaluant le délai de cicatrisation, la durée d’hospitalisation, l’aspect esthétique de la cicatrice (échelle POSAS), la fonction du MS (échelle DASH). La surface atteinte moyenne était de 3%, 4 patients avaient une atteinte circulaire. Le POSAS moyen était de 14, le DASH moyen à 6 mois de 21, s’abaissant à 11 à la dernière consultation de suivi. Le débridement enzymatique permet une rééducation plus précoce, avec des résultats fonctionnels satisfaisants. Nous pensons que cette technique est à privilégier dans le traitement hors CTB des brûlures du MS.

Published

2021

4. Glycosidases during chick embryo lung development and their colocalization with proteoglycans and growth factors

Author

G Stabellini, M Calvitti, T Baroni, L Marinucci, C Calastrini, P Carinci, and E Becchetti

Subjects

Biology (General), QH301-705.5

Abstract

During development, the epithelial component of the lung goes through a complex orderly process of branching, following strict patterns of space and time. Proteoglycans, glycosaminoglycans and growth factors are fundamental components of the extracellular matrix and perform a key role in differentiative processes. The embryonic chick lung shows a specific glycosaminoglycan composition at different levels of branching and at different embryonic stages. Proteoglycan and glycosaminoglycan accumulation is the result of secretion, absorption and degradation processes. In this pathway, enzymes, such as glycosidases, growth factors and cytokines are involved. We examined the behaviour of glycosidases, such as ß-hexosaminidases (ß-N-acetyl-D-glucosaminidase, ß- N-acetyl-D-galactosaminidase), ß-glucuronidase and ß-galactosidase, during the development of the lung bud. Our data show that the activity of the enzymes is closely linked to the processes of epithelial proliferation, bronchial tubule lengthening and infiltration of the surrounding mesenchyme. The glycosaminoglycans colocalize with transforming growth factor ß2 and inter- leukin-1 in the basement membrane and in the mesenchymal areas where the epithelium grows, and are complementary to the presence of the glycosidases. In conclusion, the activity of these glycosidases is spatially and temporally programmed and favors the release of the factors and the events which they influence.

Published

2009

5. Istologia. per le lauree magistrali e triennali

Author

D. Boni, M. Mattioli, G. Altobelli, T. Baroni, N. Bernardini, G. Bertini, C. Rosati, Bani Daniele, Boni, D., Mattioli, M., Altobelli, G., Baroni, T., Bernardini, N., Bertini, G., and Rosati, C.

Published

2019

6. Haematopoietic and stromal stem cell regulation by extracellular matrix components and growth factors

Author

M, Bodo, T, Baroni, and A, Tabilio

Subjects

Humans, Intercellular Signaling Peptides and Proteins, Bone Marrow Cells, Cell Differentiation, Stromal Cells, Hematopoietic Stem Cells, Extracellular Matrix, Hematopoiesis

Abstract

During human embryogenesis, differentiation of haematopoietic stem cells (HSCs) and their progeny is regulated spatially and temporally. In the adult, hemopoiesis is restricted to bone marrow (BM) which contains HSCs residing within the so-called 'niches'. These are microenvironments consisting of extracellular matrix (ECM) macromolecules (mainly glycosaminoglycans, proteoglycans, fibronectin and collagens) and stromal cells that act in concert to keep HSCs in quiescence or to promote their growth and differentiation, since BM stromal cells secrete specific growth factors acting on responsive stem cells. Haematopoietic precursors also secrete numerous regulatory molecules as fibroblast growth factors (FGF), interleukin 1 (IL1), and transforming growth factor-beta1 (TGFbeta1), regulating in an autocrine and/or paracrine manner the various stages of normal hematopoiesis. Although the majority of stem cells are quiescent and do nor respond to external signals, a few active stem cells responde to paracrine produced growth factors and differentiate into the more committed CD34+ haematopoietic stem cell or into a mesenchymal stem cell, which generate even more specified tissue. This review focuses on the role of both ECM molecules and growth factors that form a dynamic, interactive system crucial for lineage commitment and amplification. In this perspective, we recently described the pivotal role of ECM, FGF and TGFbeta on the GM-490 phenotype, which is a cell line established from the bone marrow of a patient with acute lymphoblastic leukemia. Our findings indicated the GM-490 cell line possess characteristics of both haematopoietic and mesenchymal precursors.

Published

2010

7. Sertoli cell-induced adult rat islet beta-cell mitogenesis: causative pathways

Author

G, Luca, M, Calvitti, T, Baroni, G, Basta, G, Angeletti, L M, Neri, E, Becchetti, S, Capitani, P, Brunetti, and R, Calafiore

Subjects

Male, Microscopy, Confocal, Sertoli Cells, Antibodies, Monoclonal, Mitosis, Proteins, Cell Count, Sensitivity and Specificity, Coculture Techniques, Rats, Rats, Sprague-Dawley, Islets of Langerhans, Diabetes Mellitus, Type 1, Glucose, Astrocytes, Culture Media, Conditioned, Insulin Secretion, Mitotic Index, Animals, Insulin, Transplantation, Homologous, Cell Division, Cells, Cultured

Abstract

We have previously observed that in vitro co-incubation of rat pre-pubertal Sertoli cells (SC), or their dialyzed/concentrated secretory products with homologous islets, resulted in significant stimulation of the islet beta-cell mitotic index. Aim of the present work was to assess both the specificity and nature of the mechanisms underlying this phenomenon. For this purpose, first we tested astrocytes (AA), separated and purified from the rat brain cortex, where they are known to release a number of growth factors and neurotrophic cytokines, for co-incubation with the islets. However, under the same experimental conditions used for SC, AA did not induce any changes in the beta-cell life cycle, thereby confirming specificity of SC, with respect to induction of beta-cell mitogenicity. For the second purpose, we examined the products of PD-1, a gene located in the cytoplasm of SC, where it promotes spermatogenesis. By blocking the protein encoded by PD-1, under appropriate culture conditions, we observed that the SC-induced increase in beta-cell mitotic activity lost its statistical significance, which suggested a role of PD-1 with respect to SC-related mitogenic properties on beta-cells. These findings corroborate the idea that SC, by either direct contact, or by means of their secretory products, clearly affect the islet beta-cell mitotic rate. Preliminarily, PD-1 gene, located in the cytoplasm of SC, might be one of the factors involved with the induction of beta-cell mitotic activity. In conclusion, SC-induced beta-cell mitotic activity is specific, seemingly mediated by humoral factors whose acting mechanisms have started being unfolded.

Published

2003

8. TGFbeta and TGFalpha, antagonistic effect in vitro on extracellular matrix accumulation by chick skin fibroblasts at two distinct embryonic stages

Author

P, Locci, T, Baroni, C, Lilli, D, Martinese, L, Marinucci, S, Bellocchio, M, Calvitti, and E, Becchetti

Subjects

Kinetics, Time Factors, Transforming Growth Factor beta, Animals, Chick Embryo, Collagen, Fibroblasts, Transforming Growth Factor alpha, Cells, Cultured, Extracellular Matrix, Fibronectins, Glycosaminoglycans

Abstract

ECM macromolecules create a specific environment that participates in the control of cell proliferation and differentiation during embryogenesis. Quantitative and qualitative alterations in the ECM may depend on several growth factors that modify cell metabolism. Since transforming growth factor beta (TGFbeta) and alpha (TGFalpha) are abundantly expressed during embryonic development in organs in which epithelial-mesenchymal interactions occur, the aim of this study was to determine: a) the effect of TGFbeta on the phenotype of 7 and 14 day chick embryo back skin (CEBS) fibroblasts by evaluating the neosynthesis of GAG, collagen and fibronectin; b) whether TGFalpha and TGFbeta production, in particular TGFbeta3 and TGFbeta4, and the number of TGFbeta receptors change during these two stages of embryonic development. The results show that the neosynthesis of ECM macromolecules, tested using radiolabelled precursors, is increased by TGFbeta. The growth factor generally favours cellular accumulation more than secretion. As far as GAG is concerned, TGFbeta has a greater stimulatory effect on sulphated GAG than on HA. Specific bioassay shows that TGFbeta3 and TGFbeta4 activity is higher in 7 day than 14 day CEBS fibroblasts. Moreover, TGFbeta3 and TGFbeta4 mRNA expression is increased in the first stages of development. Instead, the level of TGFalpha increases in successive developmental stages. Since TGFalpha stimulates the synthesis and secretion of HA, and HA binds and inactivates TGFbeta, the greater quantity of HA in 14 day fibroblasts may contribute to reducing the TGFbeta effect. Overall our data suggest that the production of TGFbeta and TGFalpha are age-dependent and that the balance between the two growth factors may be a mechanism for controlling skin differentiation.

Published

1999

9. Comparative effects of TGFbeta on proliferation of 7- and 14-day-old chick embryo fibroblasts and lack of involvement of the ODC/PA system in the TGFbeta signaling pathway

Author

R, Evangelisti, V, Valeno, G, Bosi, T, Baroni, C, Bellucci, and P, Carinci

Subjects

Eflornithine, Time Factors, Transcription, Genetic, Spermidine, Cell Cycle, Chick Embryo, Fibroblasts, Ornithine Decarboxylase, S Phase, Kinetics, Transforming Growth Factor beta, Enzyme Induction, Polyamines, Putrescine, Animals, RNA, Spermine, RNA, Messenger, Cell Division, Cells, Cultured, Signal Transduction, Skin

Abstract

The growth regulatory activity of transforming growth factor beta (TGFbeta) on chick embryo skin fibroblasts was compared in two developmental ages, days 7 and 14. The time course of 3H-thymidine incorporation, an S-phase marker of replication, was determined during 36 hr of TGFbeta treatment. Seven-day-old cells showed a prereplicative phase of 6 hr, and 14-day-old cells showed a prereplicative phase of 12 hr. DNA synthesis peaked at 24 hr in 7-day-old fibroblasts and was 10 times higher than that in 14-day-old fibroblasts. Ornithine decarboxylase (ODC) activity and content of the natural polyamines spermine (Spm), spermidine (Spd), and putrescine (Put) differed during cell cycle. ODC activity peaked at 12 hr in 7-day-old cells and at 6 hr in 14-day-old cells. Its level was two times higher at day 7 and was associated with a greater content of ODC mRNA. The maximum of polyamine (PA) concentration was determined after 12 hr of treatment in 7-day-old cells and after 36 hr in 14-day-old cells. These findings indicate that the TGFbeta proliferative response of embryo fibroblasts changes during development and is associated with activation of the ODC/PA system. Cotreatment with alpha-difluoromethylornithine, an enzyme-activated irreversible inhibitor of ODC, did not reduced growth rate. Inhibition of ODC resulted in levels of Put and Spd comparable to that of quiescent fibroblasts, whereas Spm concentration remained higher. Because an altered ODC metabolism does not convey the effects of TGFbeta on DNA synthesis, the ODC/PA system may not play a role in the pathway of TGFbeta signaling.

Published

1999

10. Downregulation of major histocompatibility complex class I expression and susceptibility to natural killer cells in cells transformed with the oncogenic adenovirus 12 are regulated by different E1A domains

Author

I, Huvent, C, Cousin, A, Kiss, M T, Baroni de Moraes, C, Bernard, and J C, D'Halluin

Subjects

Sequence Homology, Amino Acid, Histocompatibility Antigens Class I, Molecular Sequence Data, Down-Regulation, Exons, Cell Transformation, Viral, Kidney, Adenoviridae, Rats, Killer Cells, Natural, Structure-Activity Relationship, Animals, Adenovirus E1A Proteins, Amino Acid Sequence, Plasmids

Abstract

All adenoviruses transform rodent cells in vitro, but only cells transformed by serotypes belonging to subgroups A (Ad12) and B (Ad3) are tumorigenic for immunocompetent animals. In these cells, the expression of major histocompatibility complex (MHC) class I antigens is repressed and might allow them to escape from recognition by cytotoxic T lymphocytes and to develop in tumor. Furthermore, these cell lines appear resistant to lysis by natural killer (NK) cells. To determine the E1A domain(s) responsible for these properties several cell lines were created by transforming baby rat kidney cells with a set of plasmids expressing different Ad2/Ad12 hybrid E1A gene products. The class I gene expression was inhibited in cells expressing the Ad12 13S mRNA product and in cells transformed with Ad2/Ad12 hybrid E1A gene product harboring the C-terminal part of the conserved region (CR) 3 of Ad12. Susceptibility of these transformed cell lines to NK cells was determined by cytolytic assays. The results obtained suggest that two of Ad12 E1A domains are required to induce resistance of the cell lines to NK cells.

Published

1997

11. Phenotype of in vitro human otosclerotic cells and its modulation by TGF beta

Author

M, Bodo, G, Venti, T, Baroni, C, Bellucci, M, Giammarioli, E, Donti, G, Paludetti, G, Stabellini, and P, Carinci

Subjects

Otosclerosis, Phenotype, Transforming Growth Factor beta, Chondroitin Sulfates, Dermatan Sulfate, Humans, Collagen, Hyaluronic Acid, In Vitro Techniques, Bone and Bones, Cells, Cultured, Fibronectins, Glycosaminoglycans

Abstract

A study was carried out to obtain a more detailed picture of the phenotypes of human otosclerotic and normal bone cells and to analyse the response of both populations to treatment with TGF beta 1. Total collagen synthesis was found to be decreased, but fibronectin secretion increased in otosclerotic with respect to normal cells. Although overall glycosaminoglycan (GAG) synthesis was lower in otosclerotic cells, the sulphated GAG to hyaluronic acid (HA) ratio was higher, in particular there was greater expression of chondroitin (CS) and dermatan sulphates (DS). TGF beta 1 induced a more marked increase in collagen and fibronectin release and greater production of sulphated GAGs as DS and heparan sulphate (HS) in the otosclerotic cells. The fact that the phenotype of the otosclerotic cells differed from that of the normal cells and could be modified by TGF beta 1 treatment, suggests that TGF beta 1 is implicated in the pathogenesis of otosclerosis.

Published

1995

12. Internalization of Candida albicans and cytoskeletal organization in macrophages and fibroblasts treated with concanavalin A

Author

M, Bodo, E, Becchetti, T, Baroni, S, Mocci, L, Merletti, M, Giammarioli, M, Calvitti, and G, Sbaraglia

Subjects

Cell Membrane, Fluorescent Antibody Technique, Mice, Inbred Strains, Chick Embryo, Fibroblasts, Actins, Chromium Radioisotopes, Mice, Microscopy, Electron, Phagocytosis, Skin Physiological Phenomena, Candida albicans, Concanavalin A, Macrophages, Peritoneal, Animals, Actinin, Cells, Cultured, Cytoskeleton, Skin

Abstract

This paper investigates the ability of macrophages and of non-typically phagocitic cells such as fibroblasts to internalize 51Cr-labelled C. albicans in presence or in absence of lectin concanavalin A (Con A). The results obtained demonstrate that fibroblasts are also able to internalize C. albicans and that this property is potentiated by the presence of Con A. Lectin modifies only the phenotype of the fibroblast, which, poorly attached to the substrate, is globular in shape. Despite reduced cellular spreading, phagocytosis is stimulated by the lectin. In both cell populations, changes in the organization of some cytoskeletal proteins such as tubulin, actin and alpha-actinin are evident during the C. albicans infection; such rearrangements are more evident and longlasting in the fibroblasts treated with Con A.

Published

1995

13. Interleukin-1 and interleukin-6 differentially regulate the accumulation of newly synthesized extracellular matrix components and the cytokine release by developing chick embryo skin fibroblasts

Author

M, Bodo, E, Becchetti, M, Giammarioli, T, Baroni, C, Bellucci, F, Pezzetti, M, Calvitti, and P, Carinci

Subjects

Hybridomas, Interleukin-6, Chick Embryo, Thymus Gland, Fibroblasts, Extracellular Matrix, Mice, Culture Media, Conditioned, Animals, Collagen, Cell Division, Cells, Cultured, Glycosaminoglycans, Interleukin-1, Skin

Abstract

In the present study, we demonstrate that both interleukin-1 (IL-1) and interleukin-6 (IL-6) induced a significant decrease in glycosaminoglycan (GAG) synthesis and, more strikingly, secretion by 7 and 13 day-old chick embryo skin fibroblasts. We demonstrated that interleukin treatment also inhibited the synthesis of collagenase-digestible proteins (type I collagen). In addition, tissue culture supernatants (conditioned media, CM) were tested for reactivity for IL specific ELISAs and for their ability to stimulate proliferative responses in mouse thymocytes and hybridoma cells. Our findings demonstrate that chick embryo skin fibroblasts spontaneously produce IL-1 and, in even greater amounts, IL-6. Highest levels of interleukin secretion were found in the CM of 13 day-old fibroblasts and the IL-1 beta isoform was predominant over IL-1 alpha. Pretreatment of the fibroblasts with either IL-1 or IL-6 increased the secretion of both cytokines. Increased IL-1 levels were correlated with enhanced IL-1 bioactivity in the CM of IL-6 treated fibroblasts. By contrast, the raised concentrations of IL-1 in the CM of IL-1 treated cells and IL-6 in the CM of IL-1 or IL-6 treated fibroblasts failed to translate into augmented bioactivity. These observations, taken together, indicated that IL-1 and IL-6 are able to regulate the synthesis and secretion of ECM macromolecules of developing connective tissues and the cytokine release by chick embryo skin fibroblasts.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

14. Chondroitin sulphates and embryonic chick skin fibroblast proliferation

Author

M, Bodo, F, Pezzetti, M, Giammarioli, C, Bellucci, T, Baroni, and E, Becchetti

Subjects

DNA Replication, Protein Biosynthesis, Chondroitin Sulfates, Animals, Chick Embryo, DNA, Fibroblasts, Cell Division, Cells, Cultured, Culture Media, Serum-Free, Culture Media, Skin

Abstract

We have investigated the action of sulphated glycosaminoglycans (GAGs) upon primary 11-day chick embryo skin fibroblasts cultured for various periods of time in the presence or absence of fetal calf serum (FCS). Chondroitin 4- and 6-sulphate (CS) added to serum supplemented medium provoked a decrease in DNA synthesis both in sparse and crowded cultures only at high concentrations (250 micrograms/ml). Synthesis of endocellular and secreted proteins was not affected. In contrast, CS administered to fibroblasts for 24 h in serum-free medium stimulated DNA synthesis. We postulate that the CS stimulating effect seen in serum-free cultures might be antagonized by peptide regulators of cell growth normally present in serum.

Published

1994

15. Embryonic skin fibroblasts release TGF alpha and TGF beta able to influence synthesis and secretion of GAG

Author

P, Locci, C, Lilli, L, Marinucci, T, Baroni, F, Pezzetti, and E, Becchetti

Subjects

Intracellular Fluid, Epidermal Growth Factor, Drug Synergism, Chick Embryo, Fibroblasts, Transforming Growth Factor alpha, Extracellular Matrix, Gene Expression Regulation, Transforming Growth Factor beta, Culture Media, Conditioned, Animals, Cell Division, Cells, Cultured, Glycosaminoglycans, Skin

Abstract

Conditioned medium (CM), collected from 7 and 14 days-old chick embryo skin fibroblasts and added to the same cells, increases glycosaminoglycans (GAG) intra- and extracellular accumulation. The factors responsible for GAG enhancement are TGF alpha and TGF beta because they are trypsin and dithiothreitol sensitive, stable or enhanced by heat and transient acidification. Moreover, Sephadex G-75 fractions of CM active on GAG synthesis contain, when analysed on SDS-polyacrylamide gel electrophoresis, two bands that comigrate with TGF alpha and TGF beta and induce NRK cells clone 49F to form large colonies of mean size8.000 microns 2 in soft agar. Since both the factors must be present to induce the formation of large colonies we come to the conclusion that CM contains TGF alpha and TGF beta. The two growth factors have different effects on the accumulation of individual classes of GAG in the ECM. In particular, TGF beta stimulates a marked increase of CS and DS, TGF alpha of HA and DS in the medium. The contemporaneous addition of TGF alpha and TGF beta to 7 days-old fibroblasts produces a pattern of GAG response similar to CM. These embryonic fibroblasts may control their own GAG synthesis and secretion through autocrine TGF alpha and beta activity.

Published

1993

16. Cytoskeletal and DNA synthesis modification by concanavalin A in embryonic fibroblasts maintained in serum-free and serum-added medium

Author

M, Bodo, E, Becchetti, F, Pezzetti, T, Baroni, M, Calvitti, F A, Alia, and N, Arena

Subjects

Cytoskeletal Proteins, Concanavalin A, Microscopy, Electron, Scanning, Animals, Fluorescent Antibody Technique, Chick Embryo, DNA, Fibroblasts, Microtubules, Cells, Cultured, Culture Media

Abstract

The administration of lectin concanavalin A (Con A) to in vitro cultures of chick embryo fibroblasts caused dose-dependent changes in cell shape, cytoskeleton network and DNA synthesis. After 6 hrs. even a low doses of Con A produced evident effects in serum-free cultures, whereas higher doses were required to cause alterations in cells cultured in serum-added medium. As the sugar competitor mannoside abolishes the effects, it would seem that the lectin acts by binding to transmembrane receptors and that the fibronectin present in the serum engages the receptors so that they are not available to Con A.

Published

1990

17. Effects of lectins on cytoskeleton and morphology or cultured chick embryo fibroblasts

Author

N, Arena, M, Bodo, T, Baroni, F A, Alia, L, Gaspa, and E, Becchetti

Subjects

Actin Cytoskeleton, Lectins, Animals, Fluorescent Antibody Technique, Chick Embryo, Fibroblasts, Myosins, Microtubules, Actins, Cells, Cultured

Abstract

The microfilaments and microtubules of cultured chick embryo skin fibroblasts were studied in the presence of exogenous lectins by an indirect immunofluorescence technique. Lectin treatment induced modifications in the arrangement of myosin, actin and tubulin, determined depolymerization of the proteins and caused changes in cell shape and size. The results suggest that the interaction between lectins and their specific membrane receptors triggers a series of changes in the cytoskeletal pattern via transmembrana as yet unknown mechanisms and that these are responsible for the alterations in cell shape and size.

Published

1990

18. Restoration of a normal phenotype, microtubular pattern and DNA synthesis in embryonic fibroblasts concanavalin A pretreated

Author

M, Bodo, N, Arena, F, Pezzetti, T, Baroni, M, Calvitti, F A, Alia, and E, Becchetti

Subjects

Concanavalin A, Animals, Fluorescent Antibody Technique, Chick Embryo, DNA, Fibroblasts, Methylmannosides, Microtubules, Cells, Cultured, Thymidine

Abstract

The present research investigated the time required for reconstructing normal microtubular pattern and the phenotype of cells after short-term (30 min.) and long-term (24 hrs.) pretreatment with the lectin concanavalin A (Con A). Short-term pretreatment led to the formation of incomplete tubules within 2 and 24 hrs. in cells cultured in 199 medium alone. The addition of serum to the medium reversed the globular phenotype and allowed the formation of normal microtubules, even after prolonged pretreatment with Con A. Whereas long-term Con A treatment provoked a reduction in DNA synthesis in 199 alone, in serum-added 199 the percentage of 3H-thymidine incorporation of treated cells tended to reach that of controls over time.

Published

1990

19. Tricholoma niveipes

Author

T. Baroni, T. Baroni, T. Baroni, and T. Baroni

Abstract

Fungi, http://name.umdl.umich.edu/IC-HERB00IC-X-184059%5DMICH-F-184059_1, https://quod.lib.umich.edu/cgi/i/image/api/thumb/herb00ic/184059/MICH-F-184059_1/!250,250, The University of Michigan Library provides access to these materials for educational and research purposes. Some materials may be protected by copyright. If you decide to use any of these materials, you are responsible for making your own legal assessment and securing any necessary permission. If you have questions about the collection, please contact the Herbarium professional staff: herb-dlps-help@umich.edu. If you have concerns about the inclusion of an item in this collection, please contact Library Information Technology: libraryit-info@umich.edu., https://www.lib.umich.edu/about-us/policies/copyright-policy

Published

1978

20. Tricholoma niveipes

Author

T. Baroni, T. Baroni, T. Baroni, and T. Baroni

Abstract

Fungi, http://name.umdl.umich.edu/IC-HERB00IC-X-184058%5DMICH-F-184058, https://quod.lib.umich.edu/cgi/i/image/api/thumb/herb00ic/184058/MICH-F-184058/!250,250, The University of Michigan Library provides access to these materials for educational and research purposes. Some materials may be protected by copyright. If you decide to use any of these materials, you are responsible for making your own legal assessment and securing any necessary permission. If you have questions about the collection, please contact the Herbarium professional staff: herb-dlps-help@umich.edu. If you have concerns about the inclusion of an item in this collection, please contact Library Information Technology: libraryit-info@umich.edu., https://www.lib.umich.edu/about-us/policies/copyright-policy

Published

1977

21. Tricholoma manzanitae

Author

T. Baroni, T. Baroni, T. Baroni, and T. Baroni

Abstract

Fungi, http://name.umdl.umich.edu/IC-HERB00IC-X-183969%5DMICH-F-183969, https://quod.lib.umich.edu/cgi/i/image/api/thumb/herb00ic/183969/MICH-F-183969/!250,250, The University of Michigan Library provides access to these materials for educational and research purposes. Some materials may be protected by copyright. If you decide to use any of these materials, you are responsible for making your own legal assessment and securing any necessary permission. If you have questions about the collection, please contact the Herbarium professional staff: herb-dlps-help@umich.edu. If you have concerns about the inclusion of an item in this collection, please contact Library Information Technology: libraryit-info@umich.edu., https://www.lib.umich.edu/about-us/policies/copyright-policy

Published

1981

22. la divisione cellulare

Author

CARAMELLI, ELISABETTA, D. BANI T. BARONI E. BECCHETTI G. BIAGINI M. BODO LUMARE G. BRESSAN M. BUSCEMI E. CARAMELLI A. CARUSO A. GERBINO B. NICO S. PICCOLO A. PUGNALONI P. ROMAGNOLI R. SCANDROGLIO G. STABELLINI A. ZALLONE, and E. Caramelli

Subjects

CITODIERESI, FUSO MITOTICO, PIASTRA METAFASICA, CROMATIDI, CROMOSOMI

Abstract

La capacità delle cellule di dividersi è protagonista dei primi momenti della embriogenesi. A partire dallo zigote si arriva in circa 45 serie di divisioni ai 10.000 miliardi di cellule che colonizzano l'uomo adulto. La cariocinesi o mitosi si organizza in una serie ordinata di modificazioni di nucleo e citoplasma, al termine della quale si formano due cellule figlie, ciascuna delle quali contiene la stessa informazione genetica della cellula madre e la dotazione di organuli indispensabile per iniziare una vita autonoma. Nella intercinesi, o interfase, la cellula sintetizza le proteine e tutte le altre molecole necessarie per svolgere compiti specifici, inoltre si accresce ed eventualmente si prepara alla divisione successiva. Il ciclo cellulare meiotico caratterizza i gametociti e garantisce la costanza del numero di cromosomi nelle varie generazioni.

Published

2007

23. tecniche di studio in istologia

Author

CARAMELLI, ELISABETTA, D.BANI T. BARONI E.BECCHETTI G.BIAGINI M.BODO LUMARE G.BRESSAN M.BUSCEMI E.CARAMELLI A.CARUSO A.GERBINO B.NICO S.PICCOLO A.PUGNALONI P.ROMAGNOLI R. SCANDROGLIO G.STABELLINI A.ZALLONE, and E. caramelli

Abstract

il testo è imperniato sulla descrizione degli strumenti di studio in citologia ed istologia ed è corredato da una interessante iconografia finalizzata a meglio comprendere l'allestimento dei preparati e i risultati ottenibili con le varie metodiche impiegate.

Published

2007

24. Il tessuto linfoide

Author

CARAMELLI, ELISABETTA, D. BANI T. BARONI E. BECCHETTI G. BIAGINI M. BODO LUMARE G. BRESSAN M. BUSCEMI E. CARAMELLI A. CARUSO A. GERBINO B. NICO S. PICCOLO A. PUGNALONI P. ROMAGNOLI R. SCANDROGLIO G. STABELLINI A. ZALLONE, and E. CARAMELLI

Subjects

IMMUNITÀ, ANTICORPI, ORGANI LINFOIDI

Abstract

Il tessuto linfoide è una varietà di tessuto reticolare. Comprende il tessuto degli organi linfoidi (Linfonodi, milza e timo) e il tessuto linfoide associato alle mucose (MALT). Il tessuto linfoide svolge un ruolo essenziale nell'immunità.

Published

2007

25. Il nucleo

Author

CARAMELLI, ELISABETTA, D.BANI T. BARONI E.BECCHETTI G.BIAGINI M.BODO LUMARE G.BRESSAN M.BUSCEMI E.CARAMELLI A.CARUSO A.GERBINO B.NICO S.PICCOLO A.PUGNALONI P.ROMAGNOLI R. SCANDROGLIO G.STABELLINI A.ZALLONE, and e. caramelli

Subjects

INVOLUCRO NUCLEARE, LAMINA, NUCLEOLO, COMPLESSO DEL PORO, MATRICE NUCLEARE

Abstract

La presenza di una suddivisione operata dalle membrane all'interno del citoplasma rappresenta il salto evolutivo che ha portato dalla cellula procariotica a quella eucariotica. Questa compartimentazione, oltre a delimitare aree specifiche come reticolo endoplasmatico, apparato di Golgi, lisosomi e vescicole in genere, permette di segrerare il materiale genetico in un area circoscritta, il nucleo, dal resto della cellula. L'involucro nucleare, rivestito dalla lamina nucleare sul versante interno e corredato dai complessi del poro, permette al nucleo una separazione e , al tempo stesso, una comunicazione con l'ambiente extranucleare. Il materiale genetico, organizzato nella cromatina e nel nucleolo durante la fase intercinetica, ha un'organizzazione del tutto peculiare. La matrice nucleare, oltre al suo ruolo strutturale, manifesta una correlazione precisa con la distribuzione spaziale della cromatina nel nucleo e con la regolazione dell'espressione genica.

Published

2007

26. Tecniche e strumenti di studio

Author

CARAMELLI, ELISABETTA, P. CARINCI D.BANI E. BECCHETTI G. BIAGINI M. BUSCEMI E. CARAMELLI A. GERBINO B. NICO A. PUGNALONI P. ROMAGNOLI E. RUSSO BARBIERI G. STABELLINI F. TESTA RIVA A. ZALLONE, ELISABETTA CARAMELLI, E. Caramelli, P.CARINCI D.BANI T. BARONI E.BECCHETTI G.BIAGINI M. BODO LUMARE M.BUSCEMI E.CARAMELLI A.GERBINO F. GIANTOMASSI B.NICO A.PUGNALONI P.ROMAGNOLI E.RUSSO BARBIERI G.STABELLINI F.TESTA RIVA A.ZALLONE, GIANPAOLO PAPACCIO, and e.caramelli

Subjects

AUTORADIOGRAFIA, MICROSCOPIA, FRAZIONAMENTO CELLULARE, IMMUNOISTOCHIMICA, CITOFLUORIMETRIA A FLUSSO

Abstract

L'analisi morfologica permette di descrivere la forma e i rapporti tra i vari componenti della cellula. La conoscenza in questo campo è strettamente condizionata dalla progressiva disponibilità di strumentazioni innovative. Una pur elementare conoscenza degli strumenti e dei metodi di studio usati in citologia ed istologia è opportuna per una migliore comprensioni degli argomenti trattati nel testo. In breve è riportata una descrizione dei vari tipi di microscopi e di come si allestiscono i preparati istologici. Viene sottolineata la rilevanza dell'istochimica e dell'immunoistochimica.

Published

2004

27. On the Electrochemical Growth of a Crystalline p-n Junction From Aqueous Solutions.

Author

Felici R, Baroni T, Carlà F, Cioffi N, Di Benedetto F, Fontanesi C, Giaccherini A, Giurlani W, Gonidec M, Lavacchi A, Berretti E, Marcantelli P, Montegrossi G, Bonechi M, Picca RA, Poggini L, Russo F, Sportelli MC, Torsi L, and Innocenti M

Abstract

Our society largely relies on inorganic semiconductor devices which are, so far, fabricated using expensive and complex processes requiring ultra-high vacuum equipment. Here we report on the possibility of growing a p-n junction taking advantage of electrochemical processes based on the use of aqueous solutions. The growth of the junction has been carried out using the Electrochemical Atomic Layer Deposition (E-ALD) technique, which allowed to sequentially deposit two different semiconductors, CdS and Cu 2 S, on an Ag(111) substrate, in a single procedure. The growth process was monitored in situ by Surface X-Ray Diffraction (SXRD) and resulted in the fabrication of a thin double-layer structure with a high degree of crystallographic order and a well-defined interface. The high-performance electrical characteristics of the device were analysed ex-situ and show the characteristic feature of a diode., (© 2024 Wiley-VCH GmbH.)

Published

2024

28. Melatonin as a Repairing Agent in Cadmium- and Free Fatty Acid-Induced Lipotoxicity.

Author

Migni A, Mancuso F, Baroni T, Di Sante G, Rende M, Galli F, and Bartolini D

Subjects

Mice, Humans, Animals, Fatty Acids, Nonesterified, Cadmium pharmacology, Reactive Oxygen Species, Caco-2 Cells, Hepatocytes, Fatty Acids pharmacology, Palmitic Acid pharmacology, Oleic Acid pharmacology, Melatonin pharmacology, Non-alcoholic Fatty Liver Disease prevention & control

Abstract

(1) Background: Cadmium (Cd) is a potentially toxic element with a long half-life in the human body (20-40 years). Cytotoxicity mechanisms of Cd include increased levels of oxidative stress and apoptotic signaling, and recent studies have suggested that these aspects of Cd toxicity contribute a role in the pathobiology of non-alcoholic fatty liver disease (NAFLD), a highly prevalent ailment associated with hepatic lipotoxicity and an increased generation of reactive oxygen species (ROS). In this study, Cd toxicity and its interplay with fatty acid (FA)-induced lipotoxicity have been studied in intestinal epithelium and liver cells; the cytoprotective function of melatonin (MLT) has been also evaluated. (2) Methods: human liver cells (HepaRG), primary murine hepatocytes and Caco-2 intestinal epithelial cells were exposed to CdCl 2 before and after induction of lipotoxicity with oleic acid (OA) and/or palmitic acid (PA), and in some experiments, FA was combined with MLT (50 nM) treatment. (3) Results: CdCl 2 toxicity was associated with ROS induction and reduced cell viability in both the hepatic and intestinal cells. Cd and FA synergized to induce lipid droplet formation and ROS production; the latter was higher for PA compared to OA in liver cells, resulting in a higher reduction in cell viability, especially in HepaRG and primary hepatocytes, whereas CACO-2 cells showed higher resistance to Cd/PA-induced lipotoxicity compared to liver cells. MLT showed significant protection against Cd toxicity either considered alone or combined with FFA-induced lipotoxicity in primary liver cells. (4) Conclusions: Cd and PA combine their pro-oxidant activity to induce lipotoxicity in cellular populations of the gut-liver axis. MLT can be used to lessen the synergistic effect of Cd-PA on cellular ROS formation.

Published

2023

29. Sensitive peripheral nerve repair during COVID-19 emergency: does the outpatient surgical setting work as well as the operating theater?

Author

Garutti L, Tamborini F, Fagetti A, Baroni T, Bascialla E, Minini A, Cherubino M, and Valdatta L

Abstract

Background: Nerve injuries are a common occurrence among hand injuries, which at the time of the COVID-19 emergency, did not appear to have reduced their incidence. The treatment of these injuries is urgent, but the pandemic has led to a reduction in the availability of resources and a consequent reorganization of activities. Principles about Wide-Awake Local Anesthesia No Tourniquet (WALANT) in hand surgery expressed by LaLonde helped hand surgeons to adapt to this new condition by demonstrating a possible outpatient pathway for the treatment of hand traumatic conditions. In the present study, we bring our experience in nerve repair at time of COVID-19 emergency., Methods: We retrospectively enrolled in this study all patients surgically treated for a peripheral nerve injury (PNI) during the COVID-19 emergency period from March 2020 to March 2022. Demographical, anamnestic, surgical, and postoperative data were recorded and analyzed. Persisting Tinel was set as the primary outcome, while hypoesthesia and other complications as secondary outcomes., Results: Thirty-six patients have been enrolled. Despite some difference in group homogeneity in term of hypertension and multi-digital involvement, we registered no difference in term of outcomes ( P  > 0.05) between patient operated in surgical theater and in outpatient clinic and between the various techniques of nerve repair employed ( P  > 0.05)., Conclusions: Nerve repair on an outpatient facility is technically feasible and was found in this study to be safe and effective. Compared to hospitalization, the outpatient setting has a more "agile" organization and lower costs, making it preferable in selected cases.Level of evidence: Level IV, Therapeutic., Competing Interests: Competing interestsLeonardo Garutti, Federico Tamborini, Alessandro Fagetti, Tommaso Baroni, Elisa Bascialla, Andrea Minini, Mario Cherubino, and Luigi Valdatta declare no conflict of interest., (© The Author(s) 2023.)

Published

2023

30. Nickel oxide nanoparticles exposure as a risk factor for male infertility: " In vitro " effects on porcine pre-pubertal Sertoli cells.

Author

Arato I, Giovagnoli S, Di Michele A, Bellucci C, Lilli C, Aglietti MC, Bartolini D, Gambelunghe A, Muzi G, Calvitti M, Eugeni E, Gaggia F, Baroni T, Mancuso F, and Luca G

Subjects

Male, Animals, Swine, Humans, Reactive Oxygen Species metabolism, Sertoli Cells metabolism, Risk Factors, Nanoparticles, Infertility, Male

Abstract

Lately, nickel oxide nanoparticles (NiO NPs) have been employed in different industrial and biomedical fields. Several studies have reported that NiO NPs may affect the development of reproductive organs inducing oxidative stress and, resulting in male infertility. We investigated the in vitro effects of NiO NPs on porcine pre-pubertal Sertoli cells (SCs) which undergone acute (24 h) and chronic (from 1 up to 3 weeks) exposure at two subtoxic doses of NiO NPs of 1 μg/ml and 5 μg/ml. After NiO NPs exposure we performed the following analysis: (a) SCs morphological analysis (Light Microscopy); (b) ROS production and oxidative DNA damage, gene expression of antioxidant enzymes (c) SCs functionality (AMH, inhibin B Real-time PCR analysis and ELISA test); (d) apoptosis (WB analysis); (e) pro-inflammatory cytokines (Real-time PCR analysis), and (f) MAPK kinase signaling pathway (WB analysis). We found that the SCs exposed to both subtoxic doses of NiO NPs didn't sustain substantial morphological changes. NiO NPs exposure, at each concentration, reported a marked increase of intracellular ROS at the third week of treatment and DNA damage at all exposure times. We demonstrated, un up-regulation of SOD and HO-1 gene expression, at both concentrations tested. The both subtoxic doses of NiO NPs detected a down-regulation of AMH and inhibin B gene expression and secreted proteins. Only the 5 μg/ml dose induced the activation of caspase-3 at the third week. At the two subtoxic doses of NiO NPs a clear pro-inflammatory response was resulted in an up-regulation of TNF-α and IL-6 in terms of mRNA. Finally, an increased phosphorylation ratio of p-ERK1/2, p-38 and p-AKT was observed up to the third week, at both concentrations. Our results show the negative impact of subtoxic doses NiO NPs chronic exposure on porcine SCs functionality and viability., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Arato, Giovagnoli, Di Michele, Bellucci, Lilli, Aglietti, Bartolini, Gambelunghe, Muzi, Calvitti, Eugeni, Gaggia, Baroni, Mancuso and Luca.)

Published

2023

31. Zinc restores functionality in porcine prepubertal Sertoli cells exposed to subtoxic cadmium concentration via regulating the Nrf2 signaling pathway.

Author

Mancuso F, Arato I, Bellucci C, Lilli C, Eugeni E, Aglietti MC, Stabile AM, Pistilli A, Brancorsini S, Gaggia F, Calvitti M, Baroni T, and Luca G

Subjects

Male, Animals, Swine, Sertoli Cells metabolism, NF-E2-Related Factor 2 metabolism, Oxidative Stress, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction, Cadmium toxicity, Zinc metabolism

Abstract

Introduction: Among substances released into the environment by anthropogenic activities, the heavy metal cadmium (Cd) is known to induce severe testicular injury causing male subfertility/infertility. Zinc (Zn) is another heavy metal that, unlike Cd, is physiologically present in the testis, being essential for spermatogenesis. We aimed to examine the possibility that 50 µM ZnCl 2 could counteract the toxic effects induced by Cd in an in vitro model of porcine prepubertal Sertoli cells (SCs) exposed to both subtoxic (5 μM) and toxic (10 μM) concentrations of CdCl 2 for 48 h., Materials and Methods: Apoptosis, cell cycle, and cell functionality were assessed. The gene expression of Nrf2 and its downstream antioxidant enzymes, ERK1/2, and AKT kinase signaling pathways were evaluated., Materials and Results: We found that Zn, in co-treatment with subtoxic and toxic Cd concentration, increased the number of metabolically active SCs compared to Cd exposure alone but restored SC functionality only in co-treatment with subtoxic Cd concentration with respect to subtoxic Cd alone. Exposure of Cd disrupted cell cycle in SCs, and Zn co-treatment was not able to counteract this effect. Cd alone induced SC death through apoptosis and necrosis in a dose-dependent manner, and co-treatment with Zn increased the pro-apoptotic effect of Cd. Subtoxic and toxic Cd exposures activated the Nrf2 signaling pathway by increasing gene expression of Nrf2 and its downstream genes (SOD, HO-1, and GSHPx). Zn co-treatment with subtoxic Cd attenuated upregulation on the Nrf2 system, while with toxic Cd, the effect was more erratic. Studying ERK1/2 and AKT pathways as a target, we found that the phosphorylation ratio of p-ERK1/2 and p-AKT was upregulated by both subtoxic and toxic Cd exposure alone and in co-treatment with Zn., Discussion: Our results suggest that Zn could counteract Cd effects by increasing the number of metabolically active SCs, fully or partially restoring their functionality by modulating Nrf2, ERK1/2, and AKT pathways. Our SC model could be useful to study the effects of early Cd exposure on immature testis, evaluating the possible protective effects of Zn., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Mancuso, Arato, Bellucci, Lilli, Eugeni, Aglietti, Stabile, Pistilli, Brancorsini, Gaggia, Calvitti, Baroni and Luca.)

Published

2023

32. Outstation for x-ray powder diffraction at the Italian beamline at the European synchrotron.

Author

Lepore GO, Checchia S, Baroni T, Brunelli M, and d'Acapito F

Subjects

X-Ray Diffraction, Powders, Powder Diffraction, X-Rays, Synchrotrons

Abstract

LISA [Linea Italiana per la Spettroscopia di Assorbimento X, Italian beamline for X-ray Absorption Spectroscopy (XAS)] is the Italian CRG (Collaborating Research Group) beamline at the ESRF (European Synchrotron Radiation Facility) dedicated to XAS [d'Acapito et al., J. Synchrotron Radiat. 26, 551-558 (2019)]. In this work, a methodical test of the LISA beamline in performing diffraction measurements is carried out. Synchrotron x-ray diffraction measurements would complement absorption spectroscopy techniques with the long-range characterization of the material under investigation, while XAS provides the short-range element selective information.

Published

2022

33. Interplay between abiotic and microbial biofilm-mediated processes for travertine formation: Insights from a thermal spring (Piscine Carletti, Viterbo, Italy).

Author

Venturi S, Crognale S, Di Benedetto F, Montegrossi G, Casentini B, Amalfitano S, Baroni T, Rossetti S, Tassi F, Capecchiacci F, Vaselli O, and Fazi S

Subjects

Allyl Compounds, Bacteria metabolism, Biofilms, Calcium Carbonate chemistry, Calcium Sulfate chemistry, Carbon Dioxide metabolism, Minerals metabolism, Sulfides, Sulfur metabolism, Hot Springs microbiology

Abstract

Active hydrothermal travertine systems are ideal environments to investigate how abiotic and biotic processes affect mineralization mechanisms and mineral fabric formation. In this study, a biogeochemical characterization of waters, dissolved gases, and microbial mats was performed together with a mineralogical investigation on travertine encrustations occurring at the outflow channel of a thermal spring. The comprehensive model, compiled by means of TOUGHREACT computational tool from measured parameters, revealed that mineral phases were differently influenced by either abiotic conditions or microbially driven processes. Microbial mats are shaped by light availability and temperature gradient of waters flowing along the channel. Mineralogical features were homogeneous throughout the system, with euhedral calcite crystals, related to inorganic precipitation induced by CO 2 degassing, and calcite shrubs associated with organomineralization processes, thus indicating an indirect microbial participation to the mineral deposition (microbially influenced calcite). The microbial activity played a role in driving calcite redissolution processes, resulting in circular pits on calcite crystal surfaces possibly related to the metabolic activity of sulfur-oxidizing bacteria found at a high relative abundance within the biofilm community. Sulfur oxidation might also explain the occurrence of gypsum crystals embedded in microbial mats, since gypsum precipitation could be induced by a local increase in sulfate concentration mediated by S-oxidizing bacteria, regardless of the overall undersaturated environmental conditions. Moreover, the absence of gypsum dissolution suggested the capability of microbial biofilm in modulating the mobility of chemical species by providing a protective envelope on gypsum crystals., (© 2022 John Wiley & Sons Ltd.)

Published

2022

34. Effects of Titanium Dioxide Nanoparticles on Porcine Prepubertal Sertoli Cells: An " In Vitro " Study.

Author

Mancuso F, Arato I, Di Michele A, Antognelli C, Angelini L, Bellucci C, Lilli C, Boncompagni S, Fusella A, Bartolini D, Russo C, Moretti M, Nocchetti M, Gambelunghe A, Muzi G, Baroni T, Giovagnoli S, and Luca G

Subjects

Animals, Apoptosis drug effects, DNA Damage drug effects, Male, Particle Size, Sertoli Cells pathology, Signal Transduction drug effects, Sus scrofa, Metal Nanoparticles toxicity, Sertoli Cells drug effects, Titanium toxicity

Abstract

The increasing use of nanomaterials in a variety of industrial, commercial, medical products, and their environmental spreading has raised concerns regarding their potential toxicity on human health. Titanium dioxide nanoparticles (TiO 2 NPs) represent one of the most commonly used nanoparticles. Emerging evidence suggested that exposure to TiO 2 NPs induced reproductive toxicity in male animals. In this in vitro study, porcine prepubertal Sertoli cells (SCs) have undergone acute (24 h) and chronic (from 1 up to 3 weeks) exposures at both subtoxic (5 µg/ml) and toxic (100 µg/ml) doses of TiO 2 NPs. After performing synthesis and characterization of nanoparticles, we focused on SCs morphological/ultrastructural analysis, apoptosis, and functionality (AMH, inhibin B), ROS production and oxidative DNA damage, gene expression of antioxidant enzymes, proinflammatory/immunomodulatory cytokines, and MAPK kinase signaling pathway. We found that 5 µg/ml TiO 2 NPs did not induce substantial morphological changes overtime, but ultrastructural alterations appeared at the third week. Conversely, SCs exposed to 100 µg/ml TiO 2 NPs throughout the whole experiment showed morphological and ultrastructural modifications. TiO 2 NPs exposure, at each concentration, induced the activation of caspase-3 at the first and second week. AMH and inhibin B gene expression significantly decreased up to the third week at both concentrations of nanoparticles. The toxic dose of TiO 2 NPs induced a marked increase of intracellular ROS and DNA damage at all exposure times. At both concentrations, the increased gene expression of antioxidant enzymes such as SOD and HO-1 was observed whereas, at the toxic dose, a clear proinflammatory stress was evaluated along with the steady increase in the gene expression of IL-1α and IL-6. At both concentrations, an increased phosphorylation ratio of p-ERK1/2 was observed up to the second week followed by the increased phosphorylation ratio of p-NF-kB in the chronic exposure. Although in vitro , this pilot study highlights the adverse effects even of subtoxic dose of TiO 2 NPs on porcine prepubertal SCs functionality and viability and, more importantly, set the basis for further in vivo studies, especially in chronic exposure at subtoxic dose of TiO 2 NPs, a condition closer to the human exposure to this nanoagent., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Mancuso, Arato, Di Michele, Antognelli, Angelini, Bellucci, Lilli, Boncompagni, Fusella, Bartolini, Russo, Moretti, Nocchetti, Gambelunghe, Muzi, Baroni, Giovagnoli and Luca.)

Published

2022

35. Selective Enzymatic Debridement For The Management Of Acute Upper Limb Burns.

Author

Cherubino M, Valdatta L, Baroni T, Pellegatta I, Tamborini F, Garutti L, Di Summa P, and Adani R

Abstract

Upper limb burn treatment represents a major medical and surgical challenge. Enzymatic escharolysis is a rather new technique to treat thermal burns in an easy and rapid way, as an alternative to the standard of care. The aim of the study was to investigate and describe the efficacy of treatment of upper limb burns with NexoBrid® in a non-burn referral center. All patients suffering from upper limb burns and admitted within 36 hours to the Hand and Microsurgery Unit of the ASST Sette Laghi from December 2016 to June 2018 were enrolled in the study. A retrospective analysis was performed, evaluating time to wound healing, time of hospitalization, and scar aesthetic appearance with patient and observer scar assessment scale (POSAS) and disabilities of the arm, shoulder and hand score (DASH). A total of 18 patients with burns involving the upper limb from December 2016 to June 2018 were treated. The mean TBSA% involved was 3%; 4 out of 18 patients suffered circumferential burns. The mean POSAS score was 14; the mean DASH score at 6-month follow up was 21, while it reduced to 11 at the last follow up visit. Enzymatic escharolysis is a novel, rapid and selective treatment option that allows early physiotherapy with overall satisfying functional results. We believe that enzymatic escharolysis should be considered, in most cases, as the standard of care in the treatment of upper limb burn wounds in non-burn referral centers., (Copyright © 2021 Euro-Mediterranean Council for Burns and Fire Disasters.)

Published

2021

36. Social Perception of Reconstruction following Orbital Exenteration.

Author

Cherubino M, Baroni T, Santoro V, Garutti L, Battaglia P, Turri-Zanoni M, Di Summa P, Tamborini F, di Giovanna D, and Valdatta L

Abstract

Background: Orbital exenteration, the removal of the entire globe, eyelids, and orbital content, is indicated in extensive neoplastic disease involving the orbital region. Although a functional reconstruction of orbital exenteration defects is mandatory, aesthetic concerns need to be considered. Facial disfigurement following reconstructive surgery often leads to great discomfort and social retirement, which can limit social interaction. The aim of this study was to explore how the society perceives the aspect of patients who underwent orbital exenteration and subsequent reconstruction, comparing two different types of reconstruction: standard anterolateral thigh (ALT) or "sandwich" fascial ALT (SALT) free flap., Methods: An online survey was created based on four questions regarding the perception of reconstruction (discomfort at looking at that patient, perception of unhealthiness, hypothesis of social life impairment, etc); five possible answers were provided, ranging from "completely" to "not at all." The survey was administered to the general population and to medical students., Results: In total, 255 people participated to the survey (130 medical students and 125 people of the general population); a total of 245 surveys were considered eligible (10 were incomplete and then discharged). Statistical significance was found ( P < 0.001) regarding the better overall appearance of the SALT group over the ALT one., Conclusions: After analysis, the surgical outcome after SALT reconstruction has been found to be less disruptive in both groups, due to a reduced scar burden and a more pleasant orbital pocket. Our results encourage more research in the field of postexenteration reconstruction to achieve more aesthetic and social acceptability., Competing Interests: Disclosure: All the authors have no financial interest in relation to the contents of this article., (Copyright © 2021 The Authors. Published by Wolters Kluwer Health, Inc. on behalf of The American Society of Plastic Surgeons.)

Published

2021

37. Effect of EPA on Neonatal Pig Sertoli Cells " In Vitro ": A Possible Treatment to Help Maintain Fertility in Pre-Pubertal Boys Undergoing Treatment With Gonado-Toxic Therapies.

Author

Arato I, Ceccarelli V, Mancuso F, Bellucci C, Lilli C, Ferolla P, Perruccio K, D'Arpino A, Aglietti MC, Calafiore R, Cameron DF, Calvitti M, Baroni T, Vecchini A, and Luca G

Subjects

Animals, Animals, Newborn, Cancer Survivors, Cells, Cultured, Child, Cisplatin adverse effects, Eicosapentaenoic Acid therapeutic use, Fertility drug effects, Gonads drug effects, Gonads pathology, Humans, Male, Sertoli Cells cytology, Sertoli Cells physiology, Swine, Antineoplastic Combined Chemotherapy Protocols adverse effects, Eicosapentaenoic Acid pharmacology, Fertility Preservation methods, Sertoli Cells drug effects

Abstract

The incidence of cancer in pre-pubertal boys has significantly increased and, it has been recognized that the gonado-toxic effect of the cancer treatments may lead to infertility. Here, we have evaluated the effects on porcine neonatal Sertoli cells (SCs) of three commonly used chemotherapy drugs; cisplatin, 4-Hydroperoxycyclophosphamide and doxorubicin. All three drugs induced a statistical reduction of 5-hydroxymethylcytosine in comparison with the control group, performed by Immunofluorescence Analysis. The gene and protein expression levels of GDNF, were significantly down-regulated after treatment to all three chemotherapy drugs comparison with the control group. Specifically, differences in the mRNA levels of GDNF were: 0,8200 ± 0,0440, 0,6400 ± 0,0140, 0,4400 ± 0,0130 fold change at 0.33, 1.66, and 3.33μM cisplatin concentrations, respectively (**p < 0.01 at 0.33 and 1.66 μM vs SCs and ***p < 0.001 at 3.33μM vs SCs); 0,6000 ± 0,0340, 0,4200 ± 0,0130 fold change at 50 and 100 μM of 4-Hydroperoxycyclophosphamide concentrations, respectively (**p < 0.01 at both these concentrations vs SCs); 0,7000 ± 0,0340, 0,6200 ± 0,0240, 0,4000 ± 0,0230 fold change at 0.1, 0.2 and 1 µM doxorubicin concentrations, respectively (**p < 0.01 at 0.1 and 0.2 μM vs SCs and ***p < 0.001 at 1 μM vs SCs). Differences in the protein expression levels of GDNF were: 0,7400 ± 0,0340, 0,2000 ± 0,0240, 0,0400 ± 0,0230 A.U. at 0.33, 1.66, and 3.33μM cisplatin concentrations, respectively (**p < 0.01 at both these concentrations vs SCs); 0,7300 ± 0,0340, 0,4000 ± 0,0130 A.U. at 50 and 100 μM of 4- Hydroperoxycyclophosphamide concentrations, respectively (**p < 0.01 at both these concentrations vs SCs); 0,6200 ± 0,0340, 0,4000 ± 0,0240, 0,3800 ± 0,0230 A.U. at 0.l, 0.2 and 1 µM doxorubicin concentrations, respectively (**p < 0.01 at 0.1 and 0.2 μM vs SCs and ***p < 0.001 at 1 μM vs SCs). Furthermore, we have demonstrated the protective effect of eicosapentaenoic acid on SCs only at the highest concentration of cisplatin, resulting in an increase in both gene and protein expression levels of GDNF (1,3400 ± 0,0280 fold change; **p < 0.01 vs SCs); and of AMH and inhibin B that were significantly recovered with values comparable to the control group. Results from this study, offers the opportunity to develop future therapeutic strategies for male fertility management, especially in pre-pubertal boys., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Arato, Ceccarelli, Mancuso, Bellucci, Lilli, Ferolla, Perruccio, D’Arpino, Aglietti, Calafiore, Cameron, Calvitti, Baroni, Vecchini and Luca.)

Published

2021

38. Superior Helical Rim Reconstruction with a Retroauricular Perforator Transposition Flap: The Importance of a "Lifeboat" Vascular Supply.

Author

Tamborini F, Baroni T, Garutti L, Bascialla E, Valdatta L, and Cherubino M

Abstract

Competing Interests: Conflicts of Interest None declared.

Published

2021

39. Decoding overt shifts of attention in depth through pupillary and cortical frequency tagging.

Author

de'Sperati C, Roatta S, Zovetti N, and Baroni T

Subjects

Attention physiology, Electroencephalography methods, Evoked Potentials, Visual, Humans, Photic Stimulation, Pupil, User-Computer Interface, Brain-Computer Interfaces, Visual Cortex physiology

Abstract

Objective . We have recently developed a prototype of a novel human-computer interface for assistive communication based on voluntary shifts of attention (gaze) from a far target to a near target associated with a decrease of pupil size (Pupillary Accommodative Response, PAR), an automatic vegetative response that can be easily recorded. We report here an extension of that approach based on pupillary and cortical frequency tagging. Approach . In 18 healthy volunteers, we investigated the possibility of decoding attention shifts in depth by exploiting the evoked oscillatory responses of the pupil (Pupillary Oscillatory Response, POR, recorded through a low-cost device) and visual cortex (Steady-State Visual Evoked Potentials, SSVEP, recorded from 4 scalp electrodes). With a simple binary communication protocol (focusing on a far target meaning 'No', focusing on the near target meaning 'Yes'), we aimed at discriminating when observer's overt attention (gaze) shifted from the far to the near target, which were flickering at different frequencies. Main results . By applying a binary linear classifier (Support Vector Machine, SVM, with leave-one-out cross validation) to POR and SSVEP signals, we found that, with only twenty trials and no subjects' behavioural training, the offline median decoding accuracy was 75% and 80% with POR and SSVEP signals, respectively. When the two signals were combined together, accuracy reached 83%. The number of observers for whom accuracy was higher than 70% was 11/18, 12/18 and 14/18 with POR, SVVEP and combined features, respectively. A signal detection analysis confirmed these results. Significance . The present findings suggest that exploiting frequency tagging with pupillary or cortical responses during an attention shift in the depth plane, either separately or combined together, is a promising approach to realize a device for communicating with Complete Locked-In Syndrome (CLIS) patients when oculomotor control is unreliable and traditional assistive communication, even based on PAR, is unsuccessful., (© 2021 IOP Publishing Ltd.)

Published

2021

40. Anatomical Study and Clinical Application of Ulnar Artery Proximal Perforator Flaps.

Author

Cherubino M, Bolletta A, Baroni T, Di Taranto G, Losco L, Rubino C, and Valdatta L

Subjects

Dissection, Forearm surgery, Hand surgery, Humans, Perforator Flap, Plastic Surgery Procedures, Ulnar Artery surgery

Abstract

Background:  The purpose of this study is to document the vascular anatomy of the free ulnar artery proximal perforator flap and to highlight the possibility of harvesting it based on the perforators originating from the posterior ulnar recurrent artery (PURA), to spare both the main axis of vascular supply to the hand. In addition, we present a case series of five patients treated for soft tissue defects of the hand with free ulnar artery proximal perforator flaps., Methods:  Ten specimens of anterior forearm were dissected in this study to register number and characteristics of ulnar perforators. The dissection was focused on the perforators originating from the larger branch of the ulnar artery, the PURA, at the proximal third of anteromedial forearm. The anatomical dissections were evaluated in relationship with clinical dissections performed during flap harvesting in five patients., Results:  In three of the specimens dissected, the proximal perforator originated from the PURA, and in the other seven specimens, it originated directly from the ulnar artery. Five cases of reconstruction of the hand were performed with success using the free ulnar artery proximal perforator flap, and in two cases, the perforator from the PURA was found and it was possible to raise the flap based on this branch of the ulnar artery., Conclusion:  The free ulnar artery proximal perforator flap can be harvested in two different manners for the same skin island of the forearm. When possible, harvesting it form the PURA allows lengthening of the pedicle. In our experience, this flap presents many advantages such as thinness and hairlessness; it allows preservation of the ulnar neurovascular bundle with an acceptable donor site morbidity., Level of Evidence: IV., Competing Interests: None declared., (Thieme. All rights reserved.)

Published

2021

41. In "Vitro" Lps-Stimulated Sertoli Cells Pre-Loaded With Microparticles: Intracellular Activation Pathways.

Author

Arato I, Milardi D, Giovagnoli S, Grande G, Bellucci C, Lilli C, Bartoli S, Corneli S, Mazzone P, Calvitti M, Baroni T, Calafiore R, Mancuso F, and Luca G

Subjects

Animals, Animals, Newborn, Intracellular Fluid drug effects, Male, NF-kappa B metabolism, Phosphorylation drug effects, Phosphorylation physiology, Sertoli Cells drug effects, Signal Transduction drug effects, Swine, Tumor Necrosis Factor-alpha metabolism, Cell-Derived Microparticles metabolism, Intracellular Fluid metabolism, Lipopolysaccharides toxicity, Sertoli Cells metabolism, Signal Transduction physiology

Abstract

Sertoli cells (SC) are immune privileged cells with the capacity of modulating the immune response by expressing several immune-regulatory factors. SC have the capacity to respond to external stimuli through innate phagocytic and antibacterial activities. This evidence evoked a potential role of SC as drug carriers and therapeutic agents. Such stimuli drive SC towards a still unknown evolution, the clinical relevance of which as yet remains undisclosed. This study sought to investigate the effects of external stimuli in the form of polymeric microparticles (MP) and bacteria derived endotoxins, such as lipopolysaccharides (LPS), in order to identify the pathways potentially involved in cell phenotype modifications. Compared to single stimulation, when combined, MP and LPS provoked a significant increase in the gene expression of IDO, PD-L1, FAS-L, TLR-3, TLR-4, MHC-II, ICAM-1, TFGβ1, BDF123, BDF129, BDF3 and pEP2C. Western Blotting analysis demonstrated up-regulation of the ERK 1-2 and NF-kB p65 phosphorylation ratios. Our study, showing the exponential increase of these mediators upon combined MP and LPS stimulation, suggests a "switch" of SC function from typical cells of the blood-testicular barrier to nonprofessional tolerogenic antigen-presenting cells. Further studies should target the clinical and technological implications of such stimuli-induced SC transformation., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Arato, Milardi, Giovagnoli, Grande, Bellucci, Lilli, Bartoli, Corneli, Mazzone, Calvitti, Baroni, Calafiore, Mancuso and Luca.)

Published

2021

42. On the Origin of Testicular Germ Cell Tumors: From Gonocytes to Testicular Cancer.

Author

Baroni T, Arato I, Mancuso F, Calafiore R, and Luca G

Abstract

Human primordial germ cells (PGCs) have been described in the yolk sac wall around the beginning of the third week. From week 4 to 5, they migrate under control of SCF/c-KIT signaling pathway to the genital ridge, where they become gonocytes. PGCs and gonocytes express classic pluripotency markers, such as KIT, NANOG, and OCT3/4 that, during spermatogonia differentiation, are gradually suppressed, and substituted by the expression of some germ cell specific genes, such as VASA, SOX17, and TSPY. These genes, during normal development of germ cells, are tightly regulated by epigenetic modification, in terms of microRNA expression and DNA methylation. In adolescents and young adults, testicular germ cell tumors (TGCT) have a common precursor, the germ cell neoplasia in situ (GCNIS); the hypothesis of their origin from PGCs or gonocytes, whose maturation is altered, is widely accepted. The origin of TGCT, probably starting at early stages of embryogenesis, seems to be a part of the Testicular Dysgenesis Syndrome (TDS) where some early PGC/gonocytes, for still unclear reasons, are blocked in their differentiation, retaining their early marker profile. In this paper, current knowledge on the combination of epidemiological and genomic factors, involved in the development of testicular germ cell tumors, is reviewed.

Published

2019

43. Testosterone and FSH modulate Sertoli cell extracellular secretion: Proteomic analysis.

Author

Mancuso F, Calvitti M, Milardi D, Grande G, Falabella G, Arato I, Giovagnoli S, Vincenzoni F, Mancini F, Nastruzzi C, Bodo M, Baroni T, Castagnola M, Marana R, Pontecorvi A, Calafiore R, and Luca G

Subjects

Animals, Cell Separation, Extracellular Vesicles drug effects, Extracellular Vesicles metabolism, Extracellular Vesicles ultrastructure, Male, RNA, Messenger genetics, RNA, Messenger metabolism, Sertoli Cells drug effects, Swine, Follicle Stimulating Hormone pharmacology, Proteomics methods, Sertoli Cells metabolism, Testosterone pharmacology

Abstract

Spermatogenesis is a highly complicated biological process that occurs in the epithelium of the seminiferous tubules. It is regulated by a complex network of endocrine and paracrine factors and by juxtacrine testicular cross-talk. Sertoli cells (SC) play a key role in spermatogenesis due to their production of trophic, differentiation and immune-modulating factors, but many of the molecular pathways of SC action remain controversial and unclear. Over the last two decades, research has focused on extracellular vesicles as an important mechanism of intercellular communication. The aim of this study was to investigate the presence of extracellular vesicles (EVs) in SC and the modulation of their content in SC after FSH and testosterone stimulation. Highly purified porcine pre-pubertal Sertoli cells were isolated according to previously established methods. After 48 h of culture with FSH or FSH + testosterone stimulation, we identified sertolian EVs containing specific mRNAs. Proteomic analysis of EVs content identified 29 proteins under non-stimulatory conditions, most of which were related to receptor binding activity. FSH stimulation induced increases in inhibin-alpha, inhibin-beta, plakoglobin, haptoglobin, D-3-phosphoglycerate dehydrogenase and sodium/potassium-transporting ATPase in sertolian EVs. Testosterone stimulation enhanced the abundance of inhibin-alpha, inhibin-beta, tissue-type plasminogen activator, epidermal growth factor-like protein 8, elongating factor 1-gamma and D-3-phosphoglycerate dehydrogenase. These results are likely to help determine the unknown molecular secretion of Sertoli cells., (Copyright © 2018. Published by Elsevier B.V.)

Published

2018

44. Considerations and consequences of allowing DNA sequence data as types of fungal taxa.

Author

Zamora JC, Svensson M, Kirschner R, Olariaga I, Ryman S, Parra LA, Geml J, Rosling A, Adamčík S, Ahti T, Aime MC, Ainsworth AM, Albert L, Albertó E, García AA, Ageev D, Agerer R, Aguirre-Hudson B, Ammirati J, Andersson H, Angelini C, Antonín V, Aoki T, Aptroot A, Argaud D, Sosa BIA, Aronsen A, Arup U, Asgari B, Assyov B, Atienza V, Bandini D, Baptista-Ferreira JL, Baral HO, Baroni T, Barreto RW, Beker H, Bell A, Bellanger JM, Bellù F, Bemmann M, Bendiksby M, Bendiksen E, Bendiksen K, Benedek L, Bérešová-Guttová A, Berger F, Berndt R, Bernicchia A, Biketova AY, Bizio E, Bjork C, Boekhout T, Boertmann D, Böhning T, Boittin F, Boluda CG, Boomsluiter MW, Borovička J, Brandrud TE, Braun U, Brodo I, Bulyonkova T, Burdsall HH Jr, Buyck B, Burgaz AR, Calatayud V, Callac P, Campo E, Candusso M, Capoen B, Carbó J, Carbone M, Castañeda-Ruiz RF, Castellano MA, Chen J, Clerc P, Consiglio G, Corriol G, Courtecuisse R, Crespo A, Cripps C, Crous PW, da Silva GA, da Silva M, Dam M, Dam N, Dämmrich F, Das K, Davies L, De Crop E, De Kesel A, De Lange R, De Madrignac Bonzi B, Dela Cruz TEE, Delgat L, Demoulin V, Desjardin DE, Diederich P, Dima B, Dios MM, Divakar PK, Douanla-Meli C, Douglas B, Drechsler-Santos ER, Dyer PS, Eberhardt U, Ertz D, Esteve-Raventós F, Salazar JAE, Evenson V, Eyssartier G, Farkas E, Favre A, Fedosova AG, Filippa M, Finy P, Flakus A, Fos S, Fournier J, Fraiture A, Franchi P, Molano AEF, Friebes G, Frisch A, Fryday A, Furci G, Márquez RG, Garbelotto M, García-Martín JM, Otálora MAG, Sánchez DG, Gardiennet A, Garnica S, Benavent IG, Gates G, da Cruz Lima Gerlach A, Ghobad-Nejhad M, Gibertoni TB, Grebenc T, Greilhuber I, Grishkan B, Groenewald JZ, Grube M, Gruhn G, Gueidan C, Gulden G, Gusmão LF, Hafellner J, Hairaud M, Halama M, Hallenberg N, Halling RE, Hansen K, Harder CB, Heilmann-Clausen J, Helleman S, Henriot A, Hernandez-Restrepo M, Herve R, Hobart C, Hoffmeister M, Høiland K, Holec J, Holien H, Hughes K, Hubka V, Huhtinen S, Ivančević B, Jagers M, Jaklitsch W, Jansen A, Jayawardena RS, Jeppesen TS, Jeppson M, Johnston P, Jørgensen PM, Kärnefelt I, Kalinina LB, Kantvilas G, Karadelev M, Kasuya T, Kautmanová I, Kerrigan RW, Kirchmair M, Kiyashko A, Knapp DG, Knudsen H, Knudsen K, Knutsson T, Kolařík M, Kõljalg U, Košuthová A, Koszka A, Kotiranta H, Kotkova V, Koukol O, Kout J, Kovács GM, Kříž M, Kruys Å, Kučera V, Kudzma L, Kuhar F, Kukwa M, Arun Kumar TK, Kunca V, Kušan I, Kuyper TW, Lado C, Læssøe T, Lainé P, Langer E, Larsson E, Larsson KH, Laursen G, Lechat C, Lee S, Lendemer JC, Levin L, Lindemann U, Lindström H, Liu X, Hernandez RCL, Llop E, Locsmándi C, Lodge DJ, Loizides M, Lőkös L, Luangsa-Ard J, Lüderitz M, Lumbsch T, Lutz M, Mahoney D, Malysheva E, Malysheva V, Manimohan P, Marin-Felix Y, Marques G, Martínez-Gil R, Marson G, Mata G, Matheny PB, Mathiassen GH, Matočec N, Mayrhofer H, Mehrabi M, Melo I, Mešić A, Methven AS, Miettinen O, Romero AMM, Miller AN, Mitchell JK, Moberg R, Moreau PA, Moreno G, Morozova O, Morte A, Muggia L, González GM, Myllys L, Nagy I, Nagy LG, Neves MA, Niemelä T, Nimis PL, Niveiro N, Noordeloos ME, Nordin A, Noumeur SR, Novozhilov Y, Nuytinck J, Ohenoja E, Fiuza PO, Orange A, Ordynets A, Ortiz-Santana B, Pacheco L, Pál-Fám F, Palacio M, Palice Z, Papp V, Pärtel K, Pawlowska J, Paz A, Peintner U, Pennycook S, Pereira OL, Daniëls PP, Pérez-De-Gregorio Capella MÀ, Del Amo CMP, Gorjón SP, Pérez-Ortega S, Pérez-Vargas I, Perry BA, Petersen JH, Petersen RH, Pfister DH, Phukhamsakda C, Piątek M, Piepenbring M, Pino-Bodas R, Esquivel JPP, Pirot P, Popov ES, Popoff O, Álvaro MP, Printzen C, Psurtseva N, Purahong W, Quijada L, Rambold G, Ramírez NA, Raja H, Raspé O, Raymundo T, Réblová M, Rebriev YA, de Dios Reyes García J, Ripoll MÁR, Richard F, Richardson MJ, Rico VJ, Robledo GL, Barbosa FR, Rodriguez-Caycedo C, Rodriguez-Flakus P, Ronikier A, Casas LR, Rusevska K, Saar G, Saar I, Salcedo I, Martínez SMS, Montoya CAS, Sánchez-Ramírez S, Sandoval-Sierra JV, Santamaria S, Monteiro JS, Schroers HJ, Schulz B, Schmidt-Stohn G, Schumacher T, Senn-Irlet B, Ševčíková H, Shchepin O, Shirouzu T, Shiryaev A, Siepe K, Sir EB, Sohrabi M, Soop K, Spirin V, Spribille T, Stadler M, Stalpers J, Stenroos S, Suija A, Sunhede S, Svantesson S, Svensson S, Svetasheva TY, Świerkosz K, Tamm H, Taskin H, Taudière A, Tedebrand JO, Lahoz RT, Temina M, Thell A, Thines M, Thor G, Thüs H, Tibell L, Tibell S, Timdal E, Tkalčec Z, Tønsberg T, Trichies G, Triebel D, Tsurykau A, Tulloss RE, Tuovinen V, Sosa MU, Urcelay C, Valade F, Garza RV, van den Boom P, Van Vooren N, Vasco-Palacios AM, Vauras J, Velasco Santos JM, Vellinga E, Verbeken A, Vetlesen P, Vizzini A, Voglmayr H, Volobuev S, von Brackel W, Voronina E, Walther G, Watling R, Weber E, Wedin M, Weholt Ø, Westberg M, Yurchenko E, Zehnálek P, Zhang H, Zhurbenko MP, and Ekman S

Abstract

Nomenclatural type definitions are one of the most important concepts in biological nomenclature. Being physical objects that can be re-studied by other researchers, types permanently link taxonomy (an artificial agreement to classify biological diversity) with nomenclature (an artificial agreement to name biological diversity). Two proposals to amend the International Code of Nomenclature for algae, fungi, and plants (ICN), allowing DNA sequences alone (of any region and extent) to serve as types of taxon names for voucherless fungi (mainly putative taxa from environmental DNA sequences), have been submitted to be voted on at the 11 th International Mycological Congress (Puerto Rico, July 2018). We consider various genetic processes affecting the distribution of alleles among taxa and find that alleles may not consistently and uniquely represent the species within which they are contained. Should the proposals be accepted, the meaning of nomenclatural types would change in a fundamental way from physical objects as sources of data to the data themselves. Such changes are conducive to irreproducible science, the potential typification on artefactual data, and massive creation of names with low information content, ultimately causing nomenclatural instability and unnecessary work for future researchers that would stall future explorations of fungal diversity. We conclude that the acceptance of DNA sequences alone as types of names of taxa, under the terms used in the current proposals, is unnecessary and would not solve the problem of naming putative taxa known only from DNA sequences in a scientifically defensible way. As an alternative, we highlight the use of formulas for naming putative taxa (candidate taxa) that do not require any modification of the ICN.

Published

2018

45. Sertoli cells for cell transplantation: pre-clinical studies and future perspectives.

Author

Luca G, Arato I, Sorci G, Cameron DF, Hansen BC, Baroni T, Donato R, White DGJ, and Calafiore R

Subjects

Animals, Humans, Male, Sertoli Cells physiology, Sertoli Cells transplantation

Abstract

Sertoli cells are located in the testes where they control several key functions in spermatogenesis. Over the past 30 years, Sertoli cells have been upgraded from a simple scaffold-like structural system to a dynamic functional system of intercellular support that delivers potent immunomodulatory and trophic factors. Since the discovery of new Sertoli cell secretory products, these cells have been utilized in experimental cell transplantation and co-transplantation protocols aimed at treating both chronic inflammatory and degenerative disorders. For these reasons, this work reviews the application of both naked and microencapsulated Sertoli cells used in cell transplantation studies of several chronic or autoimmune diseases such as diabetes mellitus, Laron dwarfism, and Duchenne muscular dystrophy and in studies aimed at the prevention of skin allograft rejection., (© 2018 American Society of Andrology and European Academy of Andrology.)

Published

2018

46. Role of Sertoli Cell Proteins in Immunomodulation.

Author

Luca G, Baroni T, Arato I, Hansen BC, Cameron DF, and Calafiore R

Subjects

Animals, Blood-Testis Barrier cytology, Humans, Male, Sertoli Cells cytology, Blood-Testis Barrier immunology, Immune Tolerance, Sertoli Cells immunology, Spermatogenesis immunology

Abstract

Background: Sertoli cell, over the past 30 years, have been elevated from simple mechanical elements to the rank of a "sentinel" in spermatogenesis. By delivering potent immunomodulatory and trophic proteins, Sertoli cells are unique cell type with a pivotal role in maintaining testis immune privilege and the immune-protection of the antigenic germ cells., Conclusions: The findings from SC transplantation studies utilizing experimental animal models of disease, demonstrate the presence of the same immuno-modulation properties and mechanisms at tissue and organ sites far from testis. The complex pathways that generate and maintain the immune tolerance involve the production of several immunomodulatory or immune-related proteins such as cytokines, chemokines, growth factors, mediators of the inflammation, complement inhibitors or adhesion molecules. A better definition and understanding of these Sertoli cell proteins and the mechanisms of immunoprotection should help to elucidate their role in the spermatogenic process. The demonstration of their capabilities in transplantation experiments suggests that Sertoli cells may be good candidates in cell therapy for a number of cell-mediated chronic diseases., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2018

47. Xenograft of microencapsulated Sertoli cells restores glucose homeostasis in db/db mice with spontaneous diabetes mellitus.

Author

Luca G, Arato I, Mancuso F, Calvitti M, Falabella G, Murdolo G, Basta G, Cameron DF, Hansen BC, Fallarino F, Baroni T, Aglietti MC, Tortoioli C, Bodo M, and Calafiore R

Subjects

Adipose Tissue cytology, Animals, Diabetes Mellitus, Experimental, Diabetes Mellitus, Type 2 therapy, Drug Compounding, Glucose Tolerance Test methods, Heterografts immunology, Insulin Resistance physiology, Male, Mice, Transgenic, Swine, Blood Glucose metabolism, Diabetes Mellitus, Type 2 immunology, Heterografts cytology, Homeostasis immunology, Sertoli Cells transplantation, Transplantation, Heterologous methods

Abstract

Background: Increased abdominal fat and chronic inflammation in the expanded adipose tissue of obesity contribute to the development of insulin resistance and type 2 diabetes mellitus (T2D). The emerging immunoregulatory and anti-inflammatory properties of Sertoli cells have prompted their application to experimental models of autoimmune/inflammatory disorders, including diabetes. The main goal of this work was to verify whether transplantation of microencapsulated prepubertal porcine Sertoli cells (MC-SC) in the subcutaneous abdominal fat depot of spontaneously diabetic and obese db/db mice (homozygous for the diabetes spontaneous mutation [Lepr db ]) would: (i) improve glucose homeostasis and (ii) modulate local and systemic immune response and adipokines profiles., Methods: Porcine prepubertal Sertoli cells were isolated, according to previously established methods and enveloped in Barium alginate microcapsules by a mono air-jet device. MC-SC were then injected in the subcutaneous abdominal fat depot of db/db mice., Results: We have preliminarily shown that graft of MC-SC restored glucose homeostasis, with normalization of glycated hemoglobin values with improvement of the intraperitoneal glucose tolerance test in 60% of the treated animals. These results were associated with consistent increase, in the adipose tissue, of uncoupling protein 1 expression, regulatory B cells, anti-inflammatory macrophages and a concomitant decrease of proinflammatory macrophages. Furthermore, the treated animals showed a reduction in inducible NOS and proinflammatory molecules and a significant increase in an anti-inflammatory cytokine such as IL-10 along with concomitant rise of circulating adiponectin levels. The anti-hyperglycemic graft effects also emerged from an increased expression of GLUT-4, in conjunction with downregulation of GLUT-2, in skeletal muscle and liver, respectively., Conclusions: Preliminarily, xenograft of MC-SC holds promises for an effective cell therapy approach for treatment of experimental T2D., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2016

48. Computation of Femoral Canine Morphometric Parameters in Three-Dimensional Geometrical Models.

Author

Savio G, Baroni T, Concheri G, Baroni E, Meneghello R, Longo F, and Isola M

Subjects

Animals, Cadaver, Femur anatomy & histology, Dogs anatomy & histology, Femur diagnostic imaging, Imaging, Three-Dimensional veterinary, Radiography veterinary

Abstract

Objective: To define and validate a method for the measurement of 3-dimensional (3D) morphometric parameters in polygonal mesh models of canine femora., Study Design: Ex vivo/computerized model., Sample Population: Sixteen femora from 8 medium to large-breed canine cadavers (mean body weight 28.3 kg, mean age 5.3 years)., Methods: Femora were measured with a 3D scanner, obtaining 3D meshes. A computer-aided design-based (CAD) software tool was purposely developed, which allowed automatic calculation of morphometric parameters on a mesh model. Anatomic and mechanical lateral proximal femoral angles (aLPFA and mLPFA), anatomic and mechanical lateral distal femoral angles (aLDFA and mLDFA), femoral neck angle (FNA), femoral torsion angle (FTA), and femoral varus angle (FVA) were measured in 3D space. Angles were also measured onto projected planes and radiographic images., Results: Mean (SD) femoral angles (degrees) measured in 3D space were: aLPFA 115.2 (3.9), mLPFA 105.5 (4.2), aLDFA 88.6 (4.5), mLDFA 93.4 (3.9), FNA 129.6 (4.3), FTA 45 (4.5), and FVA -1.4 (4.5). Onto projection planes, aLPFA was 103.7 (5.9), mLPFA 98.4 (5.3), aLDFA 88.3 (5.5), mLDFA 93.6 (4.2), FNA 132.1 (3.5), FTA 19.1 (5.7), and FVA -1.7 (5.5). With radiographic imaging, aLPFA was 109.6 (5.9), mLPFA 105.3 (5.2), aLDFA 92.6 (3.8), mLDFA 96.9 (2.9), FNA 120.2 (8.0), FTA 30.2 (5.7), and FVA 2.6 (3.8)., Conclusion: The proposed method gives reliable and consistent information about 3D bone conformation. Results are obtained automatically and depend only on femur morphology, avoiding any operator-related bias. Angles in 3D space are different from those measured with standard radiographic methods, mainly due to the different definition of femoral axes., (© Copyright 2016 by The American College of Veterinary Surgeons.)

Published

2016

49. Long-term stability, functional competence, and safety of microencapsulated specific pathogen-free neonatal porcine Sertoli cells: a potential product for cell transplant therapy.

Author

Luca G, Mancuso F, Calvitti M, Arato I, Falabella G, Bufalari A, De Monte V, Tresoldi E, Nastruzzi C, Basta G, Fallarino F, Lilli C, Bellucci C, Baroni T, Aglietti MC, Giovagnoli S, Cameron DF, Bodo M, and Calafiore R

Subjects

Alginates, Animals, Animals, Newborn, Cell Separation, Cell Transplantation methods, Cells, Cultured, Glucuronic Acid, Hexuronic Acids, Humans, Male, Mice, Sertoli Cells cytology, Sertoli Cells physiology, Specific Pathogen-Free Organisms, Swine, Sertoli Cells transplantation, Transplantation, Heterologous methods

Abstract

Background: Porcine Sertoli cells (pSCs) have been employed for cell therapy in pre-clinical studies for several chronic/immune diseases as they deliver molecules associated with trophic and anti-inflammatory effects. To be employed for human xenografts, pSCs products need to comply with safety and stability. To fulfill such requirements, we employed a microencapsulation technology to increase pre-transplant storage stability of specific pathogen-free pSCs (SPF-pSCs) and evaluated the in vivo long-term viability and safety of grafts., Methods: Specific pathogen free neonatal pigs underwent testis excision under sterility. pSCs were isolated, characterized by immunofluorescence (IF) and cytofluorimetric analysis (CA) and examined in terms of viability and function [namely, production of anti-müllerian hormone (AMH), inhibin B, and transforming growth factor beta-1 (TFGβ-1)]. After microencapsulation in barium alginate microcapsules (Ba-MC), long-term SPF-pSCs (Ba-MCpSCs) viability and barium concentrations were evaluated at 1, 24 throughout 40 h to establish pre-transplant storage conditions., Results: The purity of isolated pSCs was about 95% with negligible contaminating cells. Cultured pSCs monolayers, both prior to and after microencapsulation, maintained high function and full viability up to 24 h of storage. At 40 h post-encapsulation, pSCs viability decreased to 80%. Barium concentration in Ba-MCpSCs lagged below the normal maximum daily allowance and was stable for 4 months in mice with no evident side effects., Conclusions: Such results suggest that this protocol for the isolation and microencapsulation of pSCs is compatible with long-haul transportation and that Ba-MCpSCs could be potentially employable for xenotransplantation., (© 2015 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2015

50. In vitro cadmium effects on ECM gene expression in human bronchial epithelial cells.

Author

Baroni T, Lilli C, Bellucci C, Luca G, Mancuso F, Fallarino F, Falabella G, Arato I, Calvitti M, Marinucci L, Muzi G, Dell'Omo M, Gambelunghe A, and Bodo M

Subjects

Apoptosis drug effects, Cell Line, Collagen genetics, Down-Regulation, Gene Expression, Humans, Integrins genetics, Metalloproteases genetics, Real-Time Polymerase Chain Reaction, Signal Transduction, Tenascin genetics, Transforming Growth Factor beta metabolism, Up-Regulation, Vitronectin genetics, Bronchi cytology, Cadmium toxicity, Epithelial Cells drug effects, Extracellular Matrix metabolism, Extracellular Matrix Proteins genetics

Abstract

Occupational and environmental exposure to the heavy metal cadmium (Cd) and its inhalation from cigarette smoke are associated with emphysema. Many growth factors and extracellular matrix (ECM) cell signaling molecules are directly involved in the epithelial bronchial cell pathway. This study investigated the direct effects of Cd on the production of several ECM components in human bronchial epithelial cells (BEAS-2B) that were exposed in vitro for 48 h to sub-toxic and toxic concentrations of Cd. Gene expression of collagens, metalloproteases (MMPs), integrins, tenascin and vitronectin were quantified by RT-PCR. To study apoptosis cascade, annexin assay and cellular cytotoxicity by MTT assay were performed. We also investigated whether an imbalance in the TGFβ/TGFβ receptor (TGFβR) expression mediated Cd effects. The results showed the sub-toxic Cd dose significantly increased tenascin, vitronectin, β1 and β5 integrin gene expression. The toxic Cd dose decreased type IV and V collagen, α1, α2 and β3 integrins. Both Cd doses down-regulated type I collagen and up-regulated metalloproteases. Each Cd dose caused a different imbalance in the complex pattern of TGFβ and its receptors. No alteration in classic apoptotic marker protein expression was observed in presence of the sub-toxic dose of Cd, suggesting this metal alters ECM production without apoptotic activation. In conclusion, all these data show even sub-toxic Cd dose exposure alters the specific gene expression of several ECM components that are crucially implicated in the mechanical properties of lung parenchyma supporting the hypothesis that the mechanism underlying Cd-induced lung disease may involve downstream changes in TGFβ/TGFβR signaling., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015